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Design, synthesis and metabolic regulation effect of farnesoid X receptor (FXR) antagonistic benzoxepin-5-ones 被引量:1

Design, synthesis and metabolic regulation effect of farnesoid X receptor (FXR) antagonistic benzoxepin-5-ones
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摘要 A series of benzoxepin-5-ones were designed and synthesized by the cyclization of chalcones which were previously found as FXR antagonists. The cellular FXR antagonism of benzoxepines was investigated,among which the most potent compound 10 l was able to reduce the plasma and hepatic triglyceride and plasma ALT levels in mice. A series of benzoxepin-5-ones were designed and synthesized by the cyclization of chalcones which were previously found as FXR antagonists. The cellular FXR antagonism of benzoxepines was investigated,among which the most potent compound 10 l was able to reduce the plasma and hepatic triglyceride and plasma ALT levels in mice.
出处 《Chinese Chemical Letters》 SCIE CAS CSCD 2017年第7期1519-1522,共4页 中国化学快报(英文版)
基金 supported by the Hong Kong,Macao and Taiwan Science & Technology Cooperation Program,MOST of China(No. 2012DFH30030)
关键词 Farnesoid X receptor Antagonist Benzoxepin-5-one Triglyceride Plasma ALT Farnesoid X receptor Antagonist Benzoxepin-5-one Triglyceride Plasma ALT
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